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ALLERGIC DISEASES. BRONCHIAL ASTHMA

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ALLERGIC DISEASES. BRONCHIAL ASTHMA EPIDEMIOLOGY Asthma is a common disease affecting 5% to 8% of the population, or about 14 to 15 million people in the USA. – PowerPoint PPT presentation

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Title: ALLERGIC DISEASES. BRONCHIAL ASTHMA


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ALLERGIC DISEASES.BRONCHIAL ASTHMA
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  • BRONCHIAL ASTHMA chronic immune inflammatory
    process with changed reactivity of bronches that
    is characterized by bronchial reactivity changes
    and has a clinical symptoms of totally reversed
    expiratory dyspnoe, asthma status or asthma
    eqiuvalents on the background of extrapulmonary
    signs of allergy, family allerig anamnesis,
    eosiniphyl rate increasing in blood and sputum.

3
EPIDEMIOLOGY
  • Asthma is a common disease affecting 5 to 8 of
    the population, or about 14 to 15 million people
    in the USA. With 5 million children afflicted, it
    is the most common chronic disease of childhood.
    Despite all we know about the pathogenesis and
    treatment of asthma, the prevalence of and
    mortality from this condition have increased.
    From 1982 to 2002 the annual age-adjusted
    prevalence rose from 34.7 to 49.4 per 1,000
    people, an increase of 42 the annual
    age-adjusted death rate for asthma rose 40 over
    this same period.Worldwide epidemiologic studies
    suggest that a large proportion of asthmatic
    people, particularly children, are also atopic.

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Allergic Sensitization
  • Allergic Sensitization -- Allergens are
    internalized by antigen-presenting cells
    (macrophages, dendritic cells, Langerhans cells)
    (A) and degraded by proteolytic enzymes in
    phagolysosomes (B), followed by intracellular
    association of allergen peptides and major
    histocompatibility complex (MHC) molecules (C).
    Complexes of MHC molecules and allergen peptides
    then move to the cell surface (D). When a T
    helper cell receptor recognizes an allergen, it
    does so by binding simultaneously to the MHC
    molecule and to the allergen partially surrounded
    by the MHC molecule (E). Interleukin-4 and other
    cytokines are then secreted by T helper cells
    (F), ultimately leading to the production of
    specific IgE by B lymphocytes (G). The specific
    IgE then attaches to mast cells and other cells
    (basophils and eosinophils), completing the
    process of sensitization (H).

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Antibody classes have distinct and overlapping
functions
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IgE complete structure
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Entire Ig structure
E
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Symptomatic Early Allergic Response
  • -- The C terminus (Fc portions) of IgE molecules
    binds avidly to mast cells and basophils through
    specific cell-surface receptors. When allergen
    molecules contact surface-bound IgE, they cause
    cross-linking of the IgE and subsequent
    degranulation of the mast cells and basophils,
    with the release of preformed mediators
    (histamine), newly generated mediators
    (prostaglandins, leukotrienes, and thromboxanes),
    and other inflammatory mediators.

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Clinical classification of bronchial asthma
  • Stage 1. Intermittent bronchial asthma
  • Clinical symptoms before treatment
  • - short-term symptoms less than once per month
  • - short-term exacerbations (several hours
    several days)
  • - night asthma symptoms less than 2 times per
    month
  • - absence of symptoms and normal lung function
    between exacerbations
  • - FEV normal,
  • decr. less 20.

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  • Stage 2. Mild-persistent bronchial asthma
  • Clinical symptoms before treatment
  • - symptoms once per day once per month
  • - exacerbations could disturb activity and
    sleeping
  • - night asthma symptoms 2-4 times per month
  • - symptoms require everyday applying of
    ß2-agonists
  • - FEV 80 of normal,
  • decr. 20-30.

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  • Stage 3. Moderate-persistent bronchial asthma
  • Clinical symptoms before treatment
  • - everyday symptoms
  • - exacerbations disturb activity and sleeping
  • - night asthma symptoms more than 1 per week
  • - symptoms require everyday applying of
    ß2-agonists
  • - FEV 60-80 of normal,
  • decr. gt 30.

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  • Stage 4. Severe-persistent bronchial asthma
  • Clinical symptoms before treatment
  • - persistent symptoms
  • - frequent exacerbations
  • - persistent night asthma symptoms
  • - symptoms require everyday applying of
    ß2-agonists, shortening of fisical activity
  • - FEV lt 60 of normal,
  • decr. gt 30.

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Key Practice Points
  • Successful implementation of specific
    environmental measures can reduce airway
    inflammation, asthma symptoms, and the need for
    medical therapy.
  • When pharmacotherapy is needed, a step-up
    approach -- based on episode severity and
    frequency -- is recommended.
  • Recent evidence suggests that specific
    immunotherapy improves asthma symptoms overall,
    with significant reductions in medication and
    bronchial hyperresponsiveness, but with only
    modest benefits on pulmonary function.

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Evaluating the Patient
  • The history. Evaluation begins with a careful
    allergy/environmental history to identify
    exposures and triggers. The clinical history
    should include (1) the nature of the
    illness/symptoms (2) precipitators and
    alleviators of symptoms (3) the frequency and
    duration of attacks (4) time lost from school or
    work (5) prior evaluation and treatment (6)
    medical history (7) family history (8) past and
    current medications and (9) occupation and
    hobbies. The environmental history should elicit
    information about these four areas
  • The home type, location, age, construction
    material number of people in residence heating
    and cooling systems (air conditioners, fans,
    dehumidifiers, humidifiers, air purifiers)
    flooring (carpets) pets (types, habitat,
    duration in residence) pests
  • The bedroom location condition types of
    bed/bedding, flooring, furniture contents of
    closets presence of window dressings and other
    dust collectors
  • General irritants smokers in the home (how many,
    smoking allowed inside?) mold or mildew use of
    aerosol sprays
  • Landscaping amount of vegetation types of
    grass, trees, flowers, shrubs exposure.

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Allergy testing.
  • Before initiating certain environmental control
    measures that may be cumbersome (eg, removing
    carpeting), expensive (eg, installing
    dehumidifiers), emotionally painful (eg, removing
    a loved pet from the home), or unnecessary (eg,
    medications or immunotherapy), it is important to
    pinpoint the allergic triggers. Allergy testing
    is the only reliable method for determining
    sensitivity to specific allergens. Its aim is to
    demonstrate allergen-specific IgE, which can be
    accomplished by skin testing or by serologic
    evaluation.

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Skin testing
  • Direct introduction of antigen into the skin of
    the patient, via the skin prick test (SPT), is
    the most common method of assessing sensitivity
    to a specific allergen. A drop of potent extract
    is placed on the skin of the volar aspect of the
    forearm or back, followed by a prick or scratch,
    which exposes the allergen to the mast cells
    located just under the stratum corneum. The
    classic wheal and flare reaction defines a
    positive test. In some cases, the SPT may be
    followed by an intracutaneous (intradermal)
    injection of extract. Compared with the SPT, the
    intradermal injection method has a higher
    sensitivity but a lower specificity. Furthermore,
    because of a larger antigen challenge, it may
    increase the risk of a systemic reaction.

20
Serologic testing
  • Certain circumstances preclude the use of skin
    testing, including extraordinary sensitivity to a
    suspected allergen, the use of antihistamines or
    ß blockers, pregnancy, dermatographism, or other
    skin abnormalities that would prevent the
    placement of the SPT. In such situations,
    serologic studies for allergy can be performed.

21
spirography
  • In addition to the history and physical
    examination, an objective measurement of lung
    function by simple pulmonary function studies
    helps to confirm a diagnosis of asthma as well as
    to establish response to therapy. The most common
    and important indices of expiratory flow are
  • Forced expiratory volume in 1 second (FEV1) the
    maximum volume of air expired in 1 second from
    full inspiration (total lung capacity TLC) to
    complete exhalation (residual volume RV) and,
  • Peak expiratory flow (PEF) the maximum flow that
    can be generated during a forced expiratory
    maneuver.
  • The forced vital capacity (FVC) maneuver (simple
    spirogram) may be graphically displayed either as
    a volume-time curve or as a flow-volume loop.

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spirography
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Making the diagnosis
  • Once allergen sensitivity is identified, it is
    important to decide on its clinical significance
    in the context of the patient's history. A
    diagnosis of allergy rests on three observations
    (1) a suggestive history with symptoms in a
    target organ such as the nose or lower
    respiratory tract (2) the demonstration of
    allergen-specific IgE and (3) the occurrence or
    aggravation of symptoms in the target organ when
    a patient is exposed to the implicated allergen.

24
Four key components of asthma therapy
  • Patient education and self-management
  • Objective assessment of lung function and disease
    severity, including home PEF monitoring
  • Environmental control with avoidance of asthma
    triggers
  • Pharmacologic therapy
  • Abbreviations PEF, peak expiratory flow

25
specific immunotherapy (SIT)
  • Identify specific allergens
  • Establish the presence of IgE antibodies
  • Confirm that symptoms emerge upon allergen
    exposure
  • Confirm the efficacy of immunotherapy for the
    specific allergens
  • Assess the severity and duration of asthma
    symptoms
  • Characterize additional triggers
  • Assess prior response to nonimmunologic therapy
  • Ascertain the availability of standardized or
    high-quality extracts
  • Assess possible contraindications to
    immunotherapy
  • Analyze sociologic factors that may affect
    immunotherapy.

26
Bronchodilators
  • Inhaled ß agonists. Short-acting inhaled
    ß-adrenergic agonists are the "rescue" agents of
    choice for symptomatic relief from acute
    bronchospasm. These agents act via a
    G-protein-linked receptor on airway smooth muscle
    cells to stimulate adenylyl cyclase and increase
    cyclic adenosine monophosphate. Beta agonists
    also inhibit mediator release from inflammatory
    cells and improve mucociliary clearance. Three
    ß2-selective agonists -- albuterol,
    metaproterenol, and terbutaline -- are among the
    most commonly used antiasthma agents (Salmeterol,
    a long-acting inhaled ß agonist, has a clinical
    effect that lasts 12 hours or more. Its long
    onset of action precludes its use as a rescue
    agent.)

27
Inhaled anticholinergics
  • Anticholinergics have been used for centuries to
    treat asthma. These drugs block the
    parasympathetic postganglionic muscarinic
    receptors found primarily in the proximal
    airways, resulting in bronchodilatation. Because
    of their low systemic absorption, inhaled
    anticholinergics such as ipratropium bromide have
    few side effects. The role of these drugs in both
    the stable and aggravated asthmatic states has
    yet to be fully defined, however.

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Theophylline
  • The use of theophylline, once a mainstay of
    asthma therapy, has waned. Although this drug is
    a useful bronchodilator, it is not as potent as
    the inhaled ß agonists. In addition, it has a
    narrow therapeutic window and its metabolism is
    affected by other drugs and disease states, which
    can make proper dosing difficult. It may be used
    as a sustained-release product for prolonged
    symptomatic relief. This drug is an option for
    some patients because of its low cost and its
    availability in oral (as opposed to inhalational)
    form.

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Cromolyn sodium and nedocromil sodium
  • These drugs exert antiinflammatory, but not
    bronchodilatory, effects. Their mechanism of
    action remains unclear, although they seem to
    inhibit the actions of a variety of inflammatory
    cells. They are useful in controlling mild to
    moderate asthma symptoms and are favored in
    children because they have few unwanted effects.

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Antileukotriene agents
  • Leukotrienes play a significant role in the
    pathogenesis of asthma. They are potent
    bronchoconstrictors, increasing airway reactivity
    in asthmatic patients and inducing an influx of
    eosinophils and neutrophils into the asthmatic
    airway. They are also potent secretagogues of
    mucus and they increase vascular permeability and
    thus airway edema. Data also support a role for
    leukotrienes in the pathogenesis of the allergic
    nasal response.20 The cysteinyl leukotrienes
    (cysLT) C4, D4, and E4 are derived from the
    metabolism of arachidonic acid by 5-lipoxygenase

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Inhaled corticosteroids
  • These are potent antiinflammatory medications
    that have a broad effect on the inflammatory
    cascade they suppress both T- and B-cell
    function inhibit inflammatory cell effector
    functions such as adhesion, chemotaxis, and
    phagocytosis and inhibit mediator production.
    Corticosteroids also up-regulate the expression
    and affinity of the ß2 receptor and thus augment
    the action of ß agonists. Systemic
    corticosteroids, unlike inhaled corticosteroids,
    are associated with many adverse effects and are
    indicated only for the management of severe
    exacerbations.

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THERAPY
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Allergists consulting is needfull
  • Is not meeting goals of therapy
  • Has moderate/severe persistent asthma
  • Has mild persistent asthma (infant or young
    child)
  • Has experienced a near-fatal asthma attack
  • Requires continuous oral corticosteroids
  • Requires frequent bursts of oral corticosteroids
  • Requires high-dose inhaled corticosteroids
  • Has atypical signs or symptoms
  • Has symptoms likely to have been precipitated by
    an occupational/environmental inhalant
  • Is a candidate for immunotherapy
  • Requires additional education about his or her
    condition
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